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Trials using anti-PD1 in recurrent glioblastoma (rGBM) have shown limited efficacy.
VEGF is a highly up-regulated pro- angiogenic growth factor in GBM , which contributes to tumor-related immunosuppression .
Preclinical data indicate that anti-vascular endothelial growth factor therapy has a potential dose effect on immune regulation.
Therefore, the combination of anti-PD1 and anti-vascular endothelial growth factor may be a promising treatment for rGBM.
Therefore, the combination of anti-PD1 and anti-vascular endothelial growth factor may be a promising treatment for rGBM.
Manmeet Singh Ahluwalia of Harvard University, et al.
randomly (1:1) 90 patients with GBM who relapsed for the first time to receive nivolumab (240 mg intravenously, the second week) and the standard dose of bevacizumab (10 mg/kg; Arm A) or low-dose (3 mg/kg; arm B) intravenously, the second week.
Stratification factors include the extent of resection, age, performance status, and MGMT methylation status.
Using CITE-seq's single-cell RNA sequencing technology, blood samples of 8 responders and 8 non-responders were analyzed before and 8 weeks after treatment.
The progression-free survival (PFS) and overall survival (OS) of the two groups of patients were compared.
They found that 90 patients (median age 60.
6 years, range 27.
4-86.
4, 67.
8% male) were enrolled between May 2018 and January 2020.
The median follow-up time for patients was 7.
7 months.
35 of the 88 patients were MGMT methylated (2 are uncertain).
There was no significant difference in overall OS between group A and group B (1 year: 41.
1 vs 37.
7%, P = 0.
14), while group A who was older than 60 years had better OS ( 1 year: 46.
2% vs 23.
8%; medium Number of digits: 10.
6 vs 5.
9 months; P = 0.
046).
For patients ≤60 years of age, there was no difference in OS between the two groups (at 1 year: 35.
6% vs 56.
4; median 8.
0 vs 12.
4 months; P = 0.
90).
The blood samples of 16 patients were analyzed by CITE-seq single-cell RNA sequencing method, baseline and 8 weeks after treatment.
Standard-dose bevacizumab-treated patients had reduced bone marrow-derived suppressor cells and inflammatory response gene characteristics at 8 weeks.
The most common toxicities (>20%) included fatigue (45.
6%), proteinuria (34.
4%), diarrhea (28.
9%), hypertension (23.
3%) and increased lipase (21.
1%).
The side effects of grade 3-4 are hypertension (7.
8%), fatigue (5.
6) and other non-neurological side effects, including deep vein thrombosis , PE, infection and abnormal liver function.
The significance of this study is that the overall PFS and OS rates of nivolumab and standard or low-dose bevacizumab appear to be similar compared to the historical benchmark of bevacizumab.
Nivolumab combined with standard bevacizumab may benefit older patients, but not younger patients.
Nivolumab combined with standard bevacizumab may benefit older patients, but not younger patients.
Nivolumab combined with standard bevacizumab may benefit older patients, but not younger patients.
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